Refolding and structural characterization of the human p53 tumor suppressor protein

Stefan Bell, Silke Hansen, Johannes Buchner

Research output: Contribution to journalArticlepeer-review

36 Scopus citations

Abstract

The human tumor suppressor p53 is a conformationally flexible and functionally complex protein that is only partially understood on a structural level. We expressed full-length p53 in the cytosol of Escherichia coli as inclusion bodies. To obtain active, recombinant p53, we varied renaturation conditions using DNA binding activity and oligomeric state as criteria for successful refolding. The optimized renaturation protocol allows the refolding of active, DNA binding p53 with correct quaternary structure and domain contact interfaces. The purified protein could be allosterically activated for DNA binding by addition of a C-terminally binding antibody. Analytical gelfiltration and chemical cross-linking confirmed the tetrameric quaternary structure and the spectroscopic analysis of renatured p53 by fluorescence and circular dichroism, suggested that native p53 is partially unstructured.

Original languageEnglish
Pages (from-to)243-257
Number of pages15
JournalBiophysical Chemistry
Volume96
Issue number2-3
DOIs
StatePublished - 2 May 2002

Keywords

  • Cancer
  • Loosely folded protein
  • Protein folding
  • Renaturation
  • p53

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